Lipoplex-mediated Transfection of Mammalian Cells Occurs through the Cholesterol-dependent Clathrin-mediated Pathway of Endocytosis

Zuhorn, Inge S.; Kalicharan, Ruby D.; Hoekstra, Dick

doi:10.1074/jbc.m111257200

Cited by 296 publications

(239 citation statements)

References 47 publications

(44 reference statements)

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“…To obtain further support for this notion, we next investigated whether correct targeting could be reestablished, after replenishment of cellular cholesterol by addition of CD/Chol complexes, as described previously (Zuhorn et al, 2002). As can be seen in Figure 9, F and G, after restoring cholesterol levels, MDR1-GFP was no longer detected at the BL membrane, displaying again its prominent presence at the BC surface, thus indicating that cholesterol is crucial for the correct AP trafficking of MDR1.…”

Section: Cholesterol Depletion Does Not Affect the Lubwx Insolubilitymentioning

confidence: 63%

“…Replenishment of depleted cholesterol was carried out by incubating the cells with preformed cyclodextrin/cholesterol complexes as described previously (Zuhorn et al, 2002). Briefly, after cholesterol depletion, HepG2 cells were washed with serum-free medium and incubated 3 h at 37°C in the presence of CD-cholesterol (CD/Chol) complexes (400 g/ml cholesterol) diluted in serum-free medium and subsequently used for cholesterol determination or for MDR1-GFP distribution.…”

Section: Miscellaneous Proceduresmentioning

confidence: 99%

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Raft-mediated Trafficking of Apical Resident Proteins Occurs in Both Direct and Transcytotic Pathways in Polarized Hepatic Cells: Role of Distinct Lipid Microdomains

Aït‐Slimane

Trugnan

IJzendoorn

et al. 2003

MBoC

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126

159

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In polarized hepatic cells, pathways and molecular principles mediating the flow of resident apical bile canalicular proteins have not yet been resolved. Herein, we have investigated apical trafficking of a glycosylphosphatidylinositol-linked and two single transmembrane domain proteins on the one hand, and two polytopic proteins on the other in polarized HepG2 cells. We demonstrate that the former arrive at the bile canalicular membrane via the indirect transcytotic pathway, whereas the polytopic proteins reach the apical membrane directly, after Golgi exit. Most importantly, cholesterol-based lipid microdomains ("rafts") are operating in either pathway, and protein sorting into such domains occurs in the biosynthetic pathway, largely in the Golgi. Interestingly, rafts involved in the direct pathway are Lubrol WX insoluble but Triton X-100 soluble, whereas rafts in the indirect pathway are both Lubrol WX and Triton X-100 insoluble. Moreover, whereas cholesterol depletion alters raft-detergent insolubility in the indirect pathway without affecting apical sorting, protein missorting occurs in the direct pathway without affecting raft insolubility. The data implicate cholesterol as a traffic direction-determining parameter in the direct apical pathway. Furthermore, raft-cargo likely distinguishing single vs. multispanning membrane anchors, rather than rafts per se (co)determine the sorting pathway.

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Section: Cholesterol Depletion Does Not Affect the Lubwx Insolubilitymentioning

confidence: 63%

Section: Miscellaneous Proceduresmentioning

confidence: 99%

Raft-mediated Trafficking of Apical Resident Proteins Occurs in Both Direct and Transcytotic Pathways in Polarized Hepatic Cells: Role of Distinct Lipid Microdomains

Aït‐Slimane

Trugnan

IJzendoorn

et al. 2003

MBoC

Self Cite

126

159

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“…39 hTF is known to be taken up via CDE while LacCer is internalized via CIE where is associated with lipid rafts. 40 Fig. S1 and S2 † show the CDE and CIE inhibitors suppressing the hTF and LacCer uptake in SHEP and HepG2 cells, respectively.…”

Section: Resultsmentioning

confidence: 99%

The endocytic pathway and therapeutic efficiency of doxorubicin conjugated cholesterol-derived polymers

et al. 2015

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Previously synthesized poly(methacrylic acid-co-cholesteryl methacrylate) P(MAA-co-CMA) copolymers were examined as potential drug delivery vehicles. P(MAA-co-CMA) copolymers were fluorescently labelled and imaged in SHEP and HepG2 cells. To understand their cell internalization pathway endocytic inhibition studies were conducted. It was concluded that P(MAA-co-CMA) are taken up by the cells via clathrin-independent endocytosis (CIE) (both caveolae mediated and cholesterol dependent endocytosis) mechanisms. The formation and characterization of P(MAA-co-CMA)-doxorubicin (DOX) nanocomplexes was investigated by fluorescence lifetime imaging microscopy (FLIM), UV-Visible spectroscopy (UV-Vis) and dynamic light scattering (DLS) studies. The toxicity screening between P(MAA-co-CMA)-DOX nanocomplexes (at varying w/w ratios) and free DOX, revealed nanocomplexes to exhibit higher cytotoxicity towards cancer cells in comparison to normal cells. FLIM and confocal microscopy were employed for investigating the time-dependent release of DOX in SHEP cells and the cellular uptake profile of P(MAAco-CMA)-DOX nanocomplexes in cancer and normal cell lines, respectively. The endocytic pathway of P(MAA-co-CMA)-DOX nanocomplexes were examined in SHEP and HepG2 cells via flow cytometry revealing the complexes to be internalized through both clathrin-dependent (CDE) and CIE mechanisms. The drug delivery profile, reported herein, illuminates the specific endocytic route and therapeutic efficiency of P(MAA-co-CMA)-DOX nanocomplexes strongly suggesting these particles to be promising candidates for in vivo applications.

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“…While several drugs that can inhibit both clathrin-and caveolae-mediated pathways of cell entry reduce transfection by SAINT-2/DOPE liposomes, HepG2 cells lack caveolae, thus implicating a clathrinmediated route in these cells. 92 Transfection by these lipoplexes could be substantially reduced by cholesterol depletion with methyl-b-cyclodextrin (MbCD) or chlorpromazine, while an inhibitor of caveolae-mediated endocytosis, 93 filipin III, blocked transfection by 20%. Localization of the lipoplexes with Tf receptor, used as a marker for clathrin-coated endosomes, 94 and inhibition of internalization by dominant-negative Eps15, and K + depletion, which both arrest coated pit formation, confirmed a clathrin-mediated route of uptake.…”

Section: Intracellular Trafficking Of Nonviral Vectors Lk Medina-kauwmentioning

confidence: 99%

“…Apparently, the size of the complex matters, as 500 nm complexes entered cells through noncoated vesicles, but not through coated vesicles, which have been reported to be 80-100 nm in diameter. 92 Importantly, complexes of this size, while able to enter cells, yielded relatively low levels of gene transfer and expression, suggesting that clathrincoated endocytosis is linked to endosomolytic ability.…”

Section: Targeted Lipopolyplexes a Ligand Which Normallymentioning

confidence: 99%

Intracellular trafficking of nonviral vectors

2005

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Lipoplex-mediated Transfection of Mammalian Cells Occurs through the Cholesterol-dependent Clathrin-mediated Pathway of Endocytosis

Cited by 296 publications

References 47 publications

Raft-mediated Trafficking of Apical Resident Proteins Occurs in Both Direct and Transcytotic Pathways in Polarized Hepatic Cells: Role of Distinct Lipid Microdomains

Raft-mediated Trafficking of Apical Resident Proteins Occurs in Both Direct and Transcytotic Pathways in Polarized Hepatic Cells: Role of Distinct Lipid Microdomains

The endocytic pathway and therapeutic efficiency of doxorubicin conjugated cholesterol-derived polymers

Intracellular trafficking of nonviral vectors

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